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首页> 外文期刊>Frontiers in Cell and Developmental Biology >Mitochondrial Quality Control Governed by Ubiquitin
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Mitochondrial Quality Control Governed by Ubiquitin

机译:由泛素治理的线粒体质量控制

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Mitochondria are essential organelles important for energy production, proliferation, and cell death. Biogenesis, homeostasis, and degradation of this organelle are tightly controlled to match cellular needs and counteract chronic stress conditions. Despite providing their own DNA, the vast majority of mitochondrial proteins are encoded in the nucleus, synthesized by cytosolic ribosomes, and subsequently imported into different mitochondrial compartments. The integrity of the mitochondrial proteome is permanently challenged by defects in folding, transport, and turnover of mitochondrial proteins. Therefore, damaged proteins are constantly sequestered from the outer mitochondrial membrane and targeted for proteasomal degradation in the cytosol via mitochondrial-associated degradation (MAD). Recent studies identified specialized quality control mechanisms important to decrease mislocalized proteins, which affect the mitochondrial import machinery. Interestingly, central factors of these ubiquitin-dependent pathways are shared with the ER-associated degradation (ERAD) machinery, indicating close collaboration between both tubular organelles. Here, we summarize recently described cellular stress response mechanisms, which are triggered by defects in mitochondrial protein import and quality control. Moreover, we discuss how ubiquitin-dependent degradation is integrated with cytosolic stress responses, particularly focused on the crosstalk between MAD and ERAD.
机译:线粒体是能源生产,增殖和细胞死亡的重要细胞器。这种细胞器的生物发生,稳态和降解被紧密控制,以匹配细胞需求并抵消慢性胁迫条件。尽管提供了自己的DNA,但绝大多数线粒体蛋白质在细胞核核糖体合成的细胞核中编码,随后进口到不同的线粒体隔室中。线粒体蛋白质组的完整性因线粒体蛋白的折叠,运输和溢出缺陷而永久性地攻击。因此,损坏的蛋白质从外部线粒体膜恒定地隔离,并且通过线粒体相关的降解(MAD)靶向胞浆中的蛋白酶体降解。最近的研究确定了对减少物质化蛋白质的专业质量控制机制,影响线粒体进口机械。有趣的是,这些泛素依赖性途径的核心因素与ER相关的降解(ERAD)机械共用,表明两个管状细胞器之间的密切合作。这里,我们概述了最近描述了细胞应激响应机制,其被线粒体蛋白质进口和质量控制的缺陷触发。此外,我们讨论了泛素依赖性降解如何与细胞溶质应激反应集成,特别是聚焦在疯狂和Erad之间的串扰上。

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